Time Series Analysis of Benzo[A]Pyrene-Induced Transcriptome Changes Suggests That a Network of Transcription Factors Regulates the Effects on Functional Gene Sets

Delft, J.H.M. van; Mathijs, Karen; Staal, Yvonne C.M.; Herwijnen, Marcel H. M. van; Brauers, Karen; Boorsma, André; Kleinjans, Jos

doi:10.1093/toxsci/kfq214

Cited by 49 publications

(70 citation statements)

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“…Recent in vitro studies have clearly illustrated the dynamic regulation occurring at the transcriptomic level during BaP exposure and the sequence of events leading to BaP toxicity [32]. Similarly, our results highlighted remarkable variations in hepatic gene transcription during pollutant exposure, with major changes occurring at 12 hours post-exposure.…”

Section: Discussionsupporting

confidence: 73%

“…The associated metabolic pathways are closely regulated by insulin or adipocytokines [39]. In our study, a significant enrichment of insulin signaling, adipocytokine signaling, glycolysis/gluconeogenesis, steroid (cholesterol) biosynthesis, and MAPK signaling pathways was observed; this may relate to late transcriptomic responses to BaP exposure in in vitro models [32]. To date, the in vivo kinetics of mechanisms regulated by BaP exposure have not been investigated.…”

Section: Discussionmentioning

confidence: 75%

“…The induction of BaP metabolism enzymes has been previously shown to occur rapidly after pollutant exposure. In the hepatic cellular model HepG2 for instance, a rapid increase in the expression of genes involved in “Dioxin, xenobiotic metabolism” was observed to drop over the first 9 hours after exposure to 751 μg.L -1 of BaP [32]. In fish exposed to a high concentration of BaP (5 mg.L -1 ), one of the main oxidases involved in phase I of the BaP metabolism process, encoded by the CYP1A gene, was over-transcribed immediately after BaP exposure with a high TR of ~ 46, decreasing to 10 6 hours post-exposure [38].…”

Section: Discussionmentioning

confidence: 99%

“…Today, this knowledge gap can be bridged using high throughput sequencing approaches, such as mRNA sequencing (mRNAseq), recovering information on gene expression over the whole transcriptome from a single experiment [28–31]. This technique has recently been shown to be more sensitive, reliable and informative than microarrays for the in vitro evaluation of BaP toxicity [32]. In the case of X. tropicalis , the interpretation of large numbers of sequences generated by mRNAseq takes advantage of the recently released complete genome [33], and benefits from a comprehensive repository from the standard model X. tropicalis, giving access to all levels of sequence data sets, including transcriptomic data [34].…”

Section: Introductionmentioning

confidence: 99%

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Impaired liver function in Xenopus tropicalis exposed to benzo[a]pyrene: transcriptomic and metabolic evidence

et al. 2014

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BackgroundDespite numerous studies suggesting that amphibians are highly sensitive to cumulative anthropogenic stresses, the role pollutants play in the decline of amphibian populations remains unclear. Amongst the most common aquatic contaminants, polycyclic aromatic hydrocarbons (PAHs) have been shown to induce several adverse effects on amphibian species in the larval stages. Conversely, adults exposed to high concentrations of the ubiquitous PAH, benzo[a]pyrene (BaP), tolerate the compound thanks to their highly efficient hepatic detoxification mechanisms. Due to this apparent lack of toxic effect on adults, no studies have examined in depth the potential toxicological impact of PAH on the physiology of adult amphibian livers. This study sheds light on the hepatic responses of Xenopus tropicalis when exposed to high environmentally relevant concentrations of BaP, by combining a high throughput transcriptomic approach (mRNA deep sequencing) and a characterization of cellular and physiological modifications to the amphibian liver.ResultsTranscriptomic changes observed in BaP-exposed Xenopus were further characterized using a time-dependent enrichment analysis, which revealed the pollutant-dependent gene regulation of important biochemical pathways, such as cholesterol biosynthesis, insulin signaling, adipocytokines signaling, glycolysis/gluconeogenesis and MAPK signaling. These results were substantiated at the physiological level with the detection of a pronounced metabolic disorder resulting in a possible insulin resistance-like syndrome phenotype. Hepatotoxicity induced by lipid and cholesterol metabolism impairments was clearly identified in BaP-exposed individuals.ConclusionsOur data suggested that BaP may disrupt overall liver physiology, and carbohydrate and cholesterol metabolism in particular, even after short-term exposure. These results are further discussed in terms of how this deregulation of liver physiology can lead to general metabolic impairment in amphibians chronically exposed to contaminants, thereby illustrating the role xenobiotics might play in the global decline in amphibian populations.Electronic supplementary materialThe online version of this article (doi:10.1186/1471-2164-15-666) contains supplementary material, which is available to authorized users.

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Section: Discussionsupporting

confidence: 73%

Section: Discussionmentioning

confidence: 75%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Impaired liver function in Xenopus tropicalis exposed to benzo[a]pyrene: transcriptomic and metabolic evidence

et al. 2014

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“…In 2010, Van Delft and colleagues generated transcription factor networks to investigate relevant transcription factors affected benzo[a]pyrene (BaP), a well-known PAH [ 30 ]. Exposure of cells to BaP (and other carcinogens) is known to alter various molecular responses, including changes in transcription factor activations.…”

Section: Network-based Analyses Of Transcriptomics Data For Exposure mentioning

confidence: 99%

Xenobiotic Metabolism Activation as a Biomarker of Cigarette Smoke Exposure Response

Iskandar

2015

Methods in Pharmacology and Toxicology

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The recent advances in "omics" technologies have generated various in silico approaches for toxicity assessment. In silico-based toxicity predictions can overcome certain major drawbacks of laboratory experiments, including the limitation of conducting experiments in a chemical-by-chemical basis that can be expensive. This chapter discusses some recent applications of in silico approaches utilizing xenobiotic metabolism that can be used to assess the impact of cigarette smoke (CS). We fi rst outline recent studies using quantum mechanics/molecular modeling and quantitative structure-activity relationships that focus on smokingrelevant cytochrome P450 (CYP) enzymes. Subsequently, we describe several network-based approaches for toxicity assessment and relevant use cases leveraging a xenobiotic metabolism network model for a quantitative assessment of CS impact.

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Concentration‐ and time‐dependent induction of Cyp1a and DNA damage response by benzo(a)pyrene in LMH three‐dimensional spheroids

Sharin

Gyasi

Jones

et al. 2021

Environ and Mol Mutagen

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In vitro liver toxicity tests performed using cell lines cultured as two‐dimensional (2D) monolayer have limited CYP450 activity and may be inadequate for screening chemicals that require activation to exert toxicity. Metabolic competence is greatly improved using three‐dimensional (3D) cell culture. In this study, Cyp1a induction, and subsequent DNA damage response induced by benzo(a)pyrene (BaP) were compared in 2D monolayer cells and 3D spheroids of the chicken hepatic cell line, LMH. Cells were exposed to BaP (0.1–100 μM) for different durations: 8, 24, 35, or 48 hr. Cyp1a activity, mRNA expression of Cyp1a and DNA damage response (DDR) genes, and phosphorylation of H2AX (γH2AX) were determined using the EROD assay, a customized PCR array, and flow cytometry, respectively. EROD activity was induced at 8 hr and achieved maximal induction at 24 hr in spheroids; earlier time points than for monolayer cells. In spheroids, BaP exposure resulted in a concentration‐dependent increase in Cyp1a4 mRNA expression at 8 hr followed by upregulation of DDR genes at 24 hr, whereas Cyp1a4 mRNA induction was only observed at 48 hr in monolayer cells. Cyp1a5 mRNA was induced at 8 hr in monolayer cells but maximum induction was greater in spheroids. An increase in γH2AX was observed at 24 hr in spheroids; this endpoint was not evaluated in monolayer cells. These results suggest that BaP metabolism precedes the DNA damage response and occurs earlier in 3D spheroids. This study demonstrates that LMH 3D spheroids could be a suitable metabolically‐competent in vitro model to measure genotoxicity of chemicals that require metabolic activation by Cyp1a.

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Time Series Analysis of Benzo[A]Pyrene-Induced Transcriptome Changes Suggests That a Network of Transcription Factors Regulates the Effects on Functional Gene Sets

Cited by 49 publications

References 61 publications

Impaired liver function in Xenopus tropicalis exposed to benzo[a]pyrene: transcriptomic and metabolic evidence

Impaired liver function in Xenopus tropicalis exposed to benzo[a]pyrene: transcriptomic and metabolic evidence

Xenobiotic Metabolism Activation as a Biomarker of Cigarette Smoke Exposure Response

Concentration‐ and time‐dependent induction of Cyp1a and DNA damage response by benzo(a)pyrene in LMH three‐dimensional spheroids

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